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Newer immunosuppressive drugs: their potential role in rheumatoid arthritis therapy.

机译:新型免疫抑制药物:它们在类风湿关节炎治疗中的潜在作用。

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摘要

Rheumatoid arthritis (RA) is a chronic immune-mediated disease characterised by chronic synovitis, which leads to cartilage damage and joint destruction. It is generally a progressive disease with radiographic evidence of joint damage, functional status decline and premature mortality. Proinflammatory cytokines, such as interleukin 1 and tumour necrosis factor alpha, play an important role in maintaining the chronicity of RA and mediating tissue damage. New approaches in the therapy of RA with anticytokine biological agents, which neutralise or block cytokines or their receptors, are now the first generation antirheumatic drugs in clinical practice. A better understanding of the signal transduction systems and gene regulation by transcription factors involved in cytokine production has opened the way for the discovery of novel therapeutic compounds useful in treating patients with RA. Overactivation of selective kinases or aberrant function of downstream transcription factors could help convert a normal immune response to a chronic disease state. This provides a unique opportunity for novel therapeutic interventions, since specific signal transduction or transcription factor targets might interrupt the perpetuation mechanisms in RA. The availability of potent and selective p38 mitogen activated protein kinase inhibitors provide a means in further dissecting the pathways implicated in cytokine production, which in turn maintain the chronicity of RA. Many studies conclude that these compounds are very useful in the treatment of chronic synovitis and therefore are very promising for RA treatment.
机译:类风湿关节炎(RA)是一种以慢性滑膜炎为特征的慢性免疫介导疾病,可导致软骨损伤和关节破坏。它通常是一种进行性疾病,具有关节损伤,功能状态下降和过早死亡的影像学证据。促炎细胞因子,例如白介素1和肿瘤坏死因子α,在维持RA的慢性和介导组织损伤中起着重要作用。中和或阻断细胞因子或其受体的抗细胞因子生物剂治疗RA的新方法现已成为临床实践中的第一代抗风湿药。通过参与细胞因子产生的转录因子对信号转导系统和基因调控的更好理解,为发现可用于治疗RA患者的新型治疗化合物开辟了道路。选择性激酶的过度激活或下游转录因子的异常功能可能有助于将正常的免疫反应转变为慢性疾病状态。这为新颖的治疗干预提供了独特的机会,因为特定的信号转导或转录因子靶标可能会干扰RA的永存机制。有效和选择性的p38丝裂原活化的蛋白激酶抑制剂的可用性为进一步剖析与细胞因子产生有关的途径提供了一种手段,这反过来又维持了RA的长期性。许多研究得出结论,这些化合物在治疗慢性滑膜炎中非常有用,因此对于RA治疗很有前景。

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